2010
DOI: 10.1016/j.neuropharm.2009.07.001
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The acute and subchronic effects of a brain-penetrating, neurotensin-1 receptor agonist on feeding, body weight and temperature

Abstract: The neurotensin-1 (NT1) receptor has been implicated in mediating a number of important neurotensin effects. We have found that PD149163, a selective, brain penetrating, NT1 receptor agonist, produces a number of therapeutic-like preclinical effects after peripheral administration including pro-cognitive, antipsychotic and anxiolytic effects. In this study, we investigated PD149163's effect on food intake and thermal regulation, two physiological processes thought to be mediated by NT1 receptor. Brown Norway r… Show more

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Cited by 47 publications
(42 citation statements)
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References 23 publications
(35 reference statements)
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“…2A), suggesting the requirement of NTS1 receptors. Because PD149163 is a small-molecule NTS1 agonist that crosses the blood-brain barrier (Feifel et al, 2004(Feifel et al, , 2010Azmi et al, 2006), we tested the effects of PD149163 on neuronal excitability recorded from stellate neurons in the EC. Bath application of PD149163 (0.25 M) robustly increased the AP firing frequency (n ϭ 10, p ϭ 0.002; Fig.…”
Section: Resultsmentioning
confidence: 99%
“…2A), suggesting the requirement of NTS1 receptors. Because PD149163 is a small-molecule NTS1 agonist that crosses the blood-brain barrier (Feifel et al, 2004(Feifel et al, , 2010Azmi et al, 2006), we tested the effects of PD149163 on neuronal excitability recorded from stellate neurons in the EC. Bath application of PD149163 (0.25 M) robustly increased the AP firing frequency (n ϭ 10, p ϭ 0.002; Fig.…”
Section: Resultsmentioning
confidence: 99%
“…In line with our previovis findings demonstrating that NTSl agonists produced potent antiallodynic effects in nerve-injured rats (21), we can thus conclude that the recruitment of both NTSl and NTS2 receptors mediates the analgesic actions of NT in chronic neuropathic pain conditions. However, since NTSl agonists were found to induce blood pressure changes and hypothermia, whereas NTS2-selective analogs did not (30,34,(72)(73)(74)(75), NTS2 analogs may therefore represent a better treatment option for painful neuropathies with a reduced side-effect profile.…”
Section: Discussionmentioning
confidence: 99%
“…ABS-201, a new acetyl-neurotensin-(8--13) analog also induces mild hypothermia in mice [12]. NT-induced hypothermia is predominantly mediated by NTS1, since NTS1 deficient mice were completely insensitive to NT [70], and PD149163, a selective NTS1 agonist, significantly lowered core body temperature in rats [71].…”
Section: Neurotensin (Nt) Systemmentioning
confidence: 99%